Cardiometabolic phenotypes and mitochondrial DNA copy number in two cohorts of UK women

Cardiometabolic phenotypes and mitochondrial DNA copy number in two cohorts of UK women

The mitochondrial genome is present at variable copy number between individuals. Mitochondria are vulnerable to oxidative stress, and their dysfunction may be associated with cardiovascular disease. The association of mitochondrial DNA copy number with cardiometabolic risk factors (lipids, glycaemic...

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Bibliographic Details
Published in:Mitochondrion Vol. 39; pp. 9 - 19
Main Authors: Guyatt, Anna L, Burrows, Kimberley, Guthrie, Philip A I, Ring, Sue, McArdle, Wendy, Day, Ian N M, Ascione, Raimondo, Lawlor, Debbie A, Gaunt, Tom R, Rodriguez, Santiago
Format: Journal Article
Language:English
Published: Netherlands Elsevier Science 01-03-2018
Subjects:
Adult
Aged
Cardiovascular Diseases - epidemiology
Cardiovascular Diseases - genetics
DNA Copy Number Variations
DNA, Mitochondrial - analysis
Female
Humans
Metabolic Diseases - epidemiology
Metabolic Diseases - genetics
Middle Aged
United Kingdom - epidemiology
United Kingdom
Cardiovascular disease
ALSPAC
Mitochondrial DNA
Diabetes
Copy number
Complex traits
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Summary:The mitochondrial genome is present at variable copy number between individuals. Mitochondria are vulnerable to oxidative stress, and their dysfunction may be associated with cardiovascular disease. The association of mitochondrial DNA copy number with cardiometabolic risk factors (lipids, glycaemic traits, inflammatory markers, anthropometry and blood pressure) was assessed in two independent cohorts of European origin women, one in whom outcomes were measured at mean (SD) age 30 (4.3) years (N=2278) and the second at 69.4 (5.5) years (N=2872). Mitochondrial DNA copy number was assayed by quantitative polymerase chain reaction. Associations were adjusted for smoking, sociodemographic status, laboratory factors and white cell traits. Out of a total of 12 outcomes assessed in both cohorts, mitochondrial DNA copy number showed little or no association with the majority (point estimates were close to zero and nearly all p-values were >0.01). The strongest evidence was for an inverse association in the older cohort with insulin (standardised beta [95%CI]: -0.06, [-0.098, -0.022], p=0.002), but this association did not replicate in the younger cohort. Our findings do not provide support for variation in mitochondrial DNA copy number having an important impact on cardio-metabolic risk factors in European origin women.
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These authors contributed equally to this work.
ISSN:1567-7249
1872-8278
DOI:10.1016/j.mito.2017.08.007